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ScharerDavid Orlando

Scharer, Orlando D.
Schärer Lab.
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Protein-protein interactions in the core nucleotide excision repair pathway

Author(s)
D'Souza, AreethaKim, MihyunChazin, Walter J.Scharer, Orlando D.
Issued Date
2024-09
DOI
10.1016/j.dnarep.2024.103728
URI
https://scholarworks.unist.ac.kr/handle/201301/83704
Citation
DNA REPAIR, v.141, pp.103728
Abstract
Nucleotide excision repair (NER) clears genomes of DNA adducts formed by UV light, environmental agents, and antitumor drugs. Gene mutations that lead to defects in the core NER reaction cause the skin cancer-prone disease xeroderma pigmentosum. . In NER, DNA lesions are excised within an oligonucleotide of 25-30 residues via a complex, multi-step reaction that is regulated by protein-protein interactions. These interactions were first characterized in the 1990s using pull-down, co-IP and yeast two-hybrid assays. More recently, high-resolution structures and detailed functional studies have started to yield detailed pictures of the progression along the NER reaction coordinate. In this review, we highlight how the study of interactions among proteins by structural and/or functional studies have provided insights into the mechanisms by which the NER machinery recognizes and excises DNA lesions. Furthermore, we identify reported, but poorly characterized or unsubstantiated interactions in need of further validation.
Publisher
ELSEVIER
ISSN
1568-7864
Keyword (Author)
Nucleotide excision repairXeroderma pigmentosumProtein-protein interactionsDNA repair
Keyword
GROUP-C PROTEINDNA-DAMAGE RECOGNITIONXERODERMA-PIGMENTOSUMCOCKAYNE-SYNDROMEXPC PROTEINMOLECULAR-MECHANISMSSTRUCTURAL BASISBINDING DOMAINDUAL INCISIONTFIIH

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